Nonapoptotic Death of Saccharomyces cerevisiae Cells That Is Stimulated by Hsp90 and Inhibited by Calcineurin and Cmk2 in Response to Endoplasmic Reticulum Stresses

doi:10.1128/EC.00291-08

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Eukaryotic Cell, December 2008, p. 2037-2051, Vol. 7, No. 12
1535-9778/08/$08.00+0 doi:10.1128/EC.00291-08
Copyright © 2008, American Society for Microbiology. All Rights Reserved.

Nonapoptotic Death of Saccharomyces cerevisiae Cells That Is Stimulated by Hsp90 and Inhibited by Calcineurin and Cmk2 in Response to Endoplasmic Reticulum Stresses

Drew D. Dudgeon, Nannan Zhang, Olufisayo O. Ositelu, Hyemin Kim, and Kyle W. Cunningham^*

Department of Biology, Johns Hopkins University, 3400 N. Charles Street, Baltimore, Maryland 21218

Received 2 September 2008/ Accepted 8 September 2008

Endoplasmic reticulum (ER) stress can trigger apoptosis andnecrosis in many types of mammalian cells. Previous studiesin yeast found little or no cell death in response to the ERstressor tunicamycin, but a recent study suggested widespreadapoptosis-like death. Here we show that wild-type laboratorySaccharomyces cerevisiae cells responding to tunicamycin dieby nonapoptotic mechanisms in low-osmolyte culture media andsurvive for long periods of time in standard synthetic media.Survival requires calcineurin, a Ca²⁺/calmodulin-dependent proteinphosphatase, but none of its known targets. The Ca²⁺/calmodulin-dependentprotein kinase Cmk2 was identified as an indirect target ofcalcineurin that suppresses death of calcineurin-deficient cells.Death of Cmk2- and/or calcineurin-deficient S. cerevisiae cellswas preceded by accumulation of reactive oxygen species butwas not associated with hallmarks of apoptosis and was not dependenton Mca1, Aif1, Nuc1, or other factors implicated in apoptosis-likedeath. Cmk2 and calcineurin also independently suppressed thedeath of S. cerevisiae cells responding to dithiothreitol ormiconazole, a common azole-class antifungal drug. Though inhibitorsof Hsp90 have been shown to diminish calcineurin signaling inS. cerevisiae and to synergistically inhibit growth in combinationwith azoles, they did not stimulate death of S. cerevisiae cellsin combination with miconazole or tunicamycin, and instead theyprevented the death of calcineurin- and Cmk2-deficient cells.These findings reveal a novel prodeath role for Hsp90 and antideathroles for calcineurin and Cmk2 that extend the life span ofS. cerevisiae cells responding to both natural and clinicalantifungal compounds.

* Corresponding author. Mailing address: Department of Biology, Johns Hopkins University, 3400 N. Charles Street, Baltimore, MD 21218. Phone: (410) 516-7844. Fax: (410) 516-5213. E-mail: kwc{at}jhu.edu

Published ahead of print on 19 September 2008.

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